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Developmental Epigenetics of the Murine Secondary Palate

机译:小鼠次Pal的发育表观遗传学。

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摘要

Orofacial clefts occur with a frequency of 1 to 2 per 1000 live births. Cleft palate, which accounts for 30% of orofacial clefts, is caused by the failure of the secondary palatal processes—medially directed, oral projections of the paired embryonic maxillary processes—to fuse. Both gene mutations and environmental effects contribute to the complex etiology of this disorder. Although much progress has been made in identifying genes whose mutations are associated with cleft palate, little is known about the mechanisms by which the environment adversely influences gene expression during secondary palate development. An increasing body of evidence, however, implicates epigenetic processes as playing a role in adversely influencing orofacial development. Epigenetics refers to inherited changes in phenotype or gene expression caused by processes other than changes in the underlying DNA sequence. Such processes include, but are not limited to, DNA methylation, microRNA effects, and histone modifications that alter chromatin conformation. In this review, we describe our current understanding of the possible role epigenetics may play during development of the secondary palate. Specifically, we present the salient features of the embryonic palatal methylome and profile the expression of numerous microRNAs that regulate protein-encoding genes crucial to normal orofacial ontogeny.
机译:口面部裂痕的发生频率为每1000例活产1至2例。 or裂占口腔颌面裂隙的30%,是由于继发pa突(成对的胚胎上颌突的中间定向,口腔突出)融合失败所致。基因突变和环境影响都导致这种疾病的复杂病因。尽管在鉴定其突变与c裂有关的基因方面已取得了很大进展,但人们对次级secondary裂发展过程中环境对基因表达产生不利影响的机理知之甚少。然而,越来越多的证据表明表观遗传过程在不利地影响口腔发育方面发挥了作用。表观遗传学是指表型或基因表达的遗传变化,是由基础DNA序列变化以外的过程引起的。此类过程包括但不限于DNA甲基化,微小RNA效应和改变染色质构象的组蛋白修饰。在这篇综述中,我们描述了我们目前对表观遗传学可能在继发development形成过程中可能扮演的角色的理解。具体来说,我们介绍了胚胎pa甲基化的显着特征,并分析了许多microRNA的表达,这些microRNA调节着对正常口面部发育至关重要的蛋白质编码基因。

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